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跨膜相互作用以及表面受体被其特异性配体封帽的机制。

Transmembrane interactions and the mechanism of capping of surface receptors by their specific ligands.

作者信息

Bourguignon L Y, Singer S J

出版信息

Proc Natl Acad Sci U S A. 1977 Nov;74(11):5031-5. doi: 10.1073/pnas.74.11.5031.

Abstract

The mechanism of capping of cell surface receptors has been examined by a double fluorescence staining procedure that permitted simultaneous observations of the distribution of a surface-bound ligand together with intracellular actin or myosin. At an early stage in the capping of the T-25 antigen or the H2 histocompatibility antigens on mouse splenic T lymphocytes, or of concanavalin A receptors on HeLa cells, when the specific receptors in question were collected into patches that were distributed over the entire cell surface, the intracellular membrane-associated actin or myosin was also accumulated into patches that were located directly under the receptor patches. These and other results have led us to propose a general molecular mechanism for the process of capping, in which actin and myosin are directly involved. It is suggested that membrane-associated actin is directly or indirectly bound to an integral protein or class of proteins, X, in the plasma membranes of eukaryotic cells. When any receptor in the membrane is aggregated by an external multivalent ligand, the aggregate binds effectively to X, whereas unaggregated receptors do not bind to X. The receptor aggregates, linked to actin (and myosin) through X, are then actively collected into a cap by an analogue of the actin--myosin sliding filament mechanism of muscle contraction.

摘要

通过双重荧光染色程序研究了细胞表面受体封帽的机制,该程序允许同时观察表面结合配体与细胞内肌动蛋白或肌球蛋白的分布情况。在小鼠脾T淋巴细胞上T-25抗原或H2组织相容性抗原封帽的早期阶段,或者在HeLa细胞上伴刀豆球蛋白A受体封帽的早期阶段,当相关的特异性受体聚集形成分布在整个细胞表面的斑块时,细胞内膜相关的肌动蛋白或肌球蛋白也会聚集形成直接位于受体斑块下方的斑块。这些结果以及其他结果使我们提出了一种封帽过程的通用分子机制,其中肌动蛋白和肌球蛋白直接参与其中。有人提出,膜相关肌动蛋白直接或间接与真核细胞质膜中的一种整合蛋白或一类蛋白X结合。当膜中的任何受体被外部多价配体聚集时,聚集体有效地与X结合,而未聚集的受体则不与X结合。通过X与肌动蛋白(和肌球蛋白)相连的受体聚集体,然后通过肌肉收缩的肌动蛋白-肌球蛋白滑动丝机制的类似物被主动收集成一个帽。

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